Mesenchymal precursor cells maintain the differentiation and proliferation potentials of breast epithelial cells.
[INTRODUCTION] Stromal-epithelial interactions play a fundamental role in tissue homeostasis, controlling cell proliferation and differentiation.
APA
Duss S, Brinkhaus H, et al. (2014). Mesenchymal precursor cells maintain the differentiation and proliferation potentials of breast epithelial cells.. Breast cancer research : BCR, 16(3), R60. https://doi.org/10.1186/bcr3673
MLA
Duss S, et al.. "Mesenchymal precursor cells maintain the differentiation and proliferation potentials of breast epithelial cells.." Breast cancer research : BCR, vol. 16, no. 3, 2014, pp. R60.
PMID
24916766
DOI
10.1186/bcr3673
Abstract
[INTRODUCTION] Stromal-epithelial interactions play a fundamental role in tissue homeostasis, controlling cell proliferation and differentiation. Not surprisingly, aberrant stromal-epithelial interactions contribute to malignancies. Studies of the cellular and molecular mechanisms underlying these interactions require ex vivo experimental model systems that recapitulate the complexity of human tissue without compromising the differentiation and proliferation potentials of human primary cells.
[METHODS] We isolated and characterized human breast epithelial and mesenchymal precursors from reduction mammoplasty tissue and tagged them with lentiviral vectors. We assembled heterotypic co-cultures and compared mesenchymal and epithelial cells to cells in corresponding monocultures by analyzing growth, differentiation potentials, and gene expression profiles.
[RESULTS] We show that heterotypic culture of non-immortalized human primary breast epithelial and mesenchymal precursors maintains their proliferation and differentiation potentials and constrains their growth. We further describe the gene expression profiles of stromal and epithelial cells in co-cultures and monocultures and show increased expression of the tumor growth factor beta (TGFβ) family member inhibin beta A (INHBA) in mesenchymal cells grown as co-cultures compared with monocultures. Notably, overexpression of INHBA in mesenchymal cells increases colony formation potential of epithelial cells, suggesting that it contributes to the dynamic reciprocity between breast mesenchymal and epithelial cells.
[CONCLUSIONS] The described heterotypic co-culture system will prove useful for further characterization of the molecular mechanisms mediating interactions between human normal or neoplastic breast epithelial cells and the stroma, and will provide a framework to test the relevance of the ever-increasing number of oncogenomic alterations identified in human breast cancer.
[METHODS] We isolated and characterized human breast epithelial and mesenchymal precursors from reduction mammoplasty tissue and tagged them with lentiviral vectors. We assembled heterotypic co-cultures and compared mesenchymal and epithelial cells to cells in corresponding monocultures by analyzing growth, differentiation potentials, and gene expression profiles.
[RESULTS] We show that heterotypic culture of non-immortalized human primary breast epithelial and mesenchymal precursors maintains their proliferation and differentiation potentials and constrains their growth. We further describe the gene expression profiles of stromal and epithelial cells in co-cultures and monocultures and show increased expression of the tumor growth factor beta (TGFβ) family member inhibin beta A (INHBA) in mesenchymal cells grown as co-cultures compared with monocultures. Notably, overexpression of INHBA in mesenchymal cells increases colony formation potential of epithelial cells, suggesting that it contributes to the dynamic reciprocity between breast mesenchymal and epithelial cells.
[CONCLUSIONS] The described heterotypic co-culture system will prove useful for further characterization of the molecular mechanisms mediating interactions between human normal or neoplastic breast epithelial cells and the stroma, and will provide a framework to test the relevance of the ever-increasing number of oncogenomic alterations identified in human breast cancer.
추출된 의학 개체 (NER)
| 유형 | 영어 표현 | 한국어 / 풀이 | UMLS CUI | 출처 | 등장 |
|---|---|---|---|---|---|
| 해부 | breast
|
유방 | dict | 6 | |
| 시술 | reduction mammoplasty
|
유방성형술 | dict | 1 | |
| 해부 | Mesenchymal precursor cells
|
scispacy | 1 | ||
| 해부 | breast epithelial cells
|
scispacy | 1 | ||
| 해부 | tissue
|
scispacy | 1 | ||
| 해부 | cell
|
scispacy | 1 | ||
| 해부 | stromal-epithelial
|
scispacy | 1 | ||
| 해부 | cellular
|
scispacy | 1 | ||
| 해부 | cells
|
scispacy | 1 | ||
| 해부 | mesenchymal
|
scispacy | 1 | ||
| 해부 | epithelial cells
|
scispacy | 1 | ||
| 해부 | stromal
|
scispacy | 1 | ||
| 해부 | co-cultures
|
scispacy | 1 | ||
| 해부 | monocultures
|
scispacy | 1 | ||
| 해부 | mesenchymal cells
|
scispacy | 1 | ||
| 해부 | stroma
|
scispacy | 1 | ||
| 약물 | [INTRODUCTION] Stromal-epithelial
|
scispacy | 1 | ||
| 질환 | human primary breast epithelial
|
scispacy | 1 | ||
| 질환 | tumor
|
C0027651
Neoplasms
|
scispacy | 1 | |
| 질환 | breast mesenchymal
|
scispacy | 1 | ||
| 질환 | breast cancer
|
C0006142
Malignant neoplasm of breast
|
scispacy | 1 | |
| 질환 | malignancies
|
scispacy | 1 | ||
| 질환 | breast epithelial
|
scispacy | 1 | ||
| 질환 | TGFβ
|
scispacy | 1 | ||
| 질환 | neoplastic breast epithelial cells
|
scispacy | 1 | ||
| 기타 | human tissue
|
scispacy | 1 | ||
| 기타 | human
|
scispacy | 1 | ||
| 기타 | human breast epithelial
|
scispacy | 1 | ||
| 기타 | lentiviral
|
scispacy | 1 | ||
| 기타 | tumor growth factor beta
|
scispacy | 1 | ||
| 기타 | inhibin beta
|
scispacy | 1 | ||
| 기타 | INHBA
→ inhibin beta A
|
scispacy | 1 | ||
| 기타 | human breast cancer
|
scispacy | 1 |
MeSH Terms
Adipocytes; Adipose Tissue; Breast; Cell Culture Techniques; Cell Differentiation; Cell Proliferation; Cells, Cultured; Coculture Techniques; Collagen Type XI; Epithelial Cells; Female; Gene Expression Profiling; Humans; Inhibin-beta Subunits; Integrin alpha Chains; Matrix Metalloproteinase 13; Mesenchymal Stem Cells; Proteoglycans; Signal Transduction; Small Leucine-Rich Proteoglycans; Transforming Growth Factor beta
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